Molecular heterogeneity assessment by next-generation sequencing and response to gefitinib of EGFR mutant advanced lung adenocarcinoma

被引：55

作者：

Bria, Emilio ^{[1
]}

Pilotto, Sara ^{[1
]}

Amato, Eliana ^{[2
]}

Fassan, Matteo ^{[2
]}

Novello, Silvia ^{[3
]}

Peretti, Umberto ^{[1
]}

Vavala, Tiziana ^{[3
]}

Kinspergher, Stefania ^{[1
]}

Righi, Luisella ^{[3
]}

Santo, Antonio ^{[1
]}

Brunelli, Matteo ^{[4
]}

Corbo, Vincenzo ^{[2
]}

Giglioli, Eliana ^{[4
]}

Sperduti, Isabella ^{[5
]}

Milella, Michele ^{[4
,6
]}

Chilosi, Marco ^{[4
]}

Scarpa, Aldo ^{[2
]}

Tortora, Giampaolo ^{[1
]}

机构：

[1] Univ Verona, Dept Med Med Oncol, Azienda Ospedaliera Univ Integrata, I-37100 Verona, Italy

[2] Univ & Azienda Osped Univ Integrata, ARC NET Ctr Appl Res Canc, Verona, Italy

[3] Univ Turin, Dept Oncol, AOU San Luigi, Turin, Italy

[4] Univ & Azienda Osped Univ Integrata, Dept Pathol & Diagnost, I-37100 Verona, Italy

[5] Regina Elena Inst Canc Res, Biostat, Rome, Italy

[6] Regina Elena Inst Canc Res, Med Oncol, Rome, Italy

来源：

ONCOTARGET | 2015年 / 6卷 / 14期

关键词：

lung cancer; EGFR; next-generation sequencing; gefitinib; TYROSINE-KINASE INHIBITORS; NONSMALL CELL LUNG; PHASE-III TRIAL; ACQUIRED-RESISTANCE; T790M MUTATIONS; CANCER; ERLOTINIB; CHEMOTHERAPY; COMBINATION; CISPLATIN;

D O I：

10.18632/oncotarget.3727

中图分类号：

R73 [肿瘤学];

学科分类号：

100214 ;

摘要：

Cancer molecular heterogeneity might explain the variable response of EGFR mutant lung adenocarcinomas to tyrosine kinase inhibitors (TKIs). We assessed the mutational status of 22 cancer genes by next-generation sequencing (NGS) in poor, intermediate or good responders to first-line gefitinib. Clinical outcome was correlated with Additional Coexisting Mutations (ACMs) and the EGFR Proportion of Mutated Alleles (PMA). Thirteen ACMs were found in 10/17 patients: TP53 (n=6), KRAS (n=2), CTNNB1 (n=2), PIK3CA, SMAD4 and MET (n=1 each). TP53 mutations were exclusive of poor/intermediate responders (66.7% versus 0, p=0.009). Presence of ACMs significantly affected both PFS (median 3.0 versus 12.3 months, p=0.03) and survival (3.6 months versus not reached, p=0.03). TP53 mutation was the strongest negative modifier (median PFS 4.0 versus 14.0 months). Higher EGFR PMA was present in good versus poor/intermediate responders. Median PFS and survival were longer in patients with EGFR PMA >= 0.36 (12.0 versus 4.0 months, p=0.31; not reached versus 18.0 months, p=0.59). Patients with an EGFR PMA >= 0.36 and no ACMs fared significantly better (p=0.03), with a trend towards increased survival (p=0.06). Our exploratory data suggest that a quantitative (PMA) and qualitative (ACMs) molecular heterogeneity assessment using NGS might be useful for a better selection of patients.

引用

页码：12783 / 12795

页数：13

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